Development and validation of a multigene variant profiling assay to guide targeted and immuno therapy selection in solid tumors

Development and validation of a multigene variant profiling assay to guide targeted and immuno therapy selection in solid tumors

We present data on analytical validation of the multigene variant profiling assay (CellDx) to provide actionable indications for selection of targeted and immune checkpoint inhibitor (ICI) therapy in solid tumors. CellDx includes Next Generation Sequencing (NGS) profiling of gene variants in a targe...

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Bibliographic Details
Published in:PloS one Vol. 16; no. 2; p. e0246048
Main Authors: Akolkar, Dadasaheb, Patil, Darshana, Srivastava, Navin, Patil, Revati, Datta, Vineet, Apurwa, Sachin, Yashwante, Nitin, Dhasarathan, Raja, Gosavi, Rahul, John, Jinumary, Khan, Shabishta, Jadhav, Ninad, Mene, Priti, Ahire, Dhanashri, Pawar, Sushant, Bodke, Harshal, Sahoo, Subhraline, Nile, Arun, Saindane, Dinesh, Darokar, Harshal, Devhare, Pradip, Srinivasan, Ajay, Datar, Rajan
Format: Journal Article
Language:English
Published: United States Public Library of Science 08-02-2021
Public Library of Science (PLoS)
Subjects:
Abnormalities
Amplification
Aneuploidy
Biochemical assays
Biology and Life Sciences
Cancer
Capillary electrophoresis
Carcinogenesis
Carcinogens
Data analysis
Deoxyribonucleic acid
DNA
DNA sequencing
Drug therapy
Editing
Electrophoresis
Epidermal growth factor
Epidermal growth factor receptors
Ethics
FDA approval
Gene fusion
Genes
Genetic aspects
Genetic variation
Genetics
Genomics
Growth factors
Immune checkpoint inhibitors
Immunotherapy
Kinases
Lung cancer
Lung diseases
Medical research
Medicine and Health Sciences
Methodology
Methods
Microsatellite instability
Mismatch repair
MLH1 protein
Molecular targeted therapy
Monoclonal antibodies
MSH2 protein
MSH6 protein
Mutation
Nucleotide sequencing
Oncology, Experimental
Paraffin
Paraffins
Patients
PD-L1 protein
Pembrolizumab
Protein-tyrosine kinase
Research and analysis methods
Reviews
Ribonucleic acid
RNA
Software
Solid tumors
Targeted cancer therapy
Tumors
Tyrosine
Visualization
India
United States > US
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Description
Summary:We present data on analytical validation of the multigene variant profiling assay (CellDx) to provide actionable indications for selection of targeted and immune checkpoint inhibitor (ICI) therapy in solid tumors. CellDx includes Next Generation Sequencing (NGS) profiling of gene variants in a targeted 452-gene panel as well as status of total Tumor Mutation Burden (TMB), Microsatellite instability (MSI), Mismatch Repair (MMR) and Programmed Cell Death-Ligand 1 (PD-L1) respectively. Validation parameters included accuracy, sensitivity, specificity and reproducibility for detection of Single Nucleotide Alterations (SNAs), Copy Number Alterations (CNAs), Insertions and Deletions (Indels), Gene fusions, MSI and PDL1. Cumulative analytical sensitivity and specificity of the assay were 99.03 (95% CI: 96.54-99.88) and 99.23% (95% CI: 98.54% - 99.65%) respectively with 99.20% overall Accuracy (95% CI: 98.57% - 99.60%) and 99.7% Precision based on evaluation of 116 reference samples. The clinical performance of CellDx was evaluated in a subsequent analysis of 299 clinical samples where 861 unique mutations were detected of which 791 were oncogenic and 47 were actionable. Indications in MMR, MSI and TMB for selection of ICI therapies were also detected in the clinical samples. The high specificity, sensitivity, accuracy and reproducibility of the CellDx assay is suitable for clinical application for guiding selection of targeted and immunotherapy agents in patients with solid organ tumors.
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Competing Interests: I have read the journal’s policy and the authors of this manuscript have the following competing interests: All author except RD2 are employees of the Funding Institution, i.e., Datar Cancer Genetics (DCG), which offers commercial services in oncology. RD2 is the founder and Managing Director of the Funding Institution, and holds patents on products in development as well as marketed products which incorporate technology described in this manuscript as well as other similar technologies. This does not alter our adherence to PLOS ONE policies on sharing data and materials.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0246048